Host Cell Rab GTPases in Hepatitis B Virus Infection

Zeyen, Lisa; Prange, Reinhild

doi:10.3389/fcell.2018.00154

Cited by 20 publications

(17 citation statements)

References 79 publications

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“…Supernatants of HBV-transfected HepAD38 cells harbored predominantly defective naked capsids, which were reported to exit stable HBV-transfected cells via an alternative secretion pathway compared to virions. 18 In contrast, infected HepG2-NTCPsec+ released high levels of LHBs-enveloped virions but no detectable naked capsids. An excess of secreted naked capsids is likely an aberrant product of transfected hepatoma cells where HBV replication is driven by chromosomally integrated HBV DNA, exhibiting epigenetic regulation distinct from that of viral replication driven by episomal cccDNA in infected cells.…”

Section: Discussionmentioning

confidence: 94%

Efficient long-term amplification of hepatitis B virus isolates after infection of slow proliferating HepG2-NTCP cells

König

Yang

et al. 2019

Journal of Hepatology

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Cell culture system that mimicks complete HBV life cycle from entry to egress.Efficient in vitro infection with crude HBV patient sera.Up to 50-and 1,300-fold net amplification of patient-and cell culture-derived input HBV in the supernatant.Polyethylene glycol-independent HBV spread to adjacent cells, forming infected cell clusters.Evaluation of patient-and cell culture-derived HBV amplification w/wo antivirals over 8 weeks.

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Section: Discussionmentioning

confidence: 94%

Efficient long-term amplification of hepatitis B virus isolates after infection of slow proliferating HepG2-NTCP cells

König

Yang

et al. 2019

Journal of Hepatology

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“…The majority of HBsAg is incorporated into subviral particles that are formed at the ER membrane, not at the multivesicular bodies, and outnumber virions by more than a thousand‐fold (Patient et al., 2007; Tong & Revill, 2016). The secretion of subviral particles occurs via the Golgi network and the constitutive secretion pathway (Zeyen & Prange, 2018). Only a minority of HBV envelopes are transported to multivesicular bodies via uncharacterized pathways for complete virion formation.…”

Section: Discussionmentioning

confidence: 99%

Efficient and reproducible depletion of hepatitis B virus from plasma derived extracellular vesicles

Jung

Jacobs

Avalbaev

et al. 2020

J of Extracellular Vesicle

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Extracellular vesicles (EVs) are emerging fundamental players in viral infections by shuttling viral components, mediating immune responses and likely the spread of the virus. However, the obstacles involved in purifying EVs and removing contaminating viral particles in a reliable and effective manner bottlenecks the full potential for the development of clinical and diagnostic treatment options targeting EV. Because of the similarities in size, density, membrane composition and mode of biogenesis of EVs and virions there are no standardized approaches for virus‐removal from EV preparations yet. Functional EV studies also require EV samples that are devoid of antibody contaminants. Consequently, the study of EVs in virology needs reliable and effective protocols to purify EVs and remove contaminating antibodies and viral particles. Here, we established a protocol for EV purification from hepatitis B virus (HBV)‐containing plasma by a combination of size‐exclusion chromatography and affinity‐based purification. After purification, EV samples were free of virus‐sized particles, HBV surface antigen, HBV core antigen, antibodies or infectious material. Viral genomic contamination was also decreased following purification. By using appropriate antibodies and size parameters, this protocol could potentially be applied to purification of EVs from other viral samples. In summary, we established a fast, reproducible and robust approach for the removal of HBV from EV preparations. Looking forward to the point of purifying EVs from clinical samples, this method should enable studies shedding light on the underlying mechanisms of EVs in viral infections and their diagnostic and prognostic potential.

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“…The Rab family of small GTPases are fundamental to intracellular membrane trafficking in which organelles exchange proteins and lipids in an intricate network of vesicular transport. Furthermore, many viral and bacterial pathogens exploit Rabs for entry and survival [2][3][4][5][6] , and Rab misregulation is associated with human diseases such as neurodegeneration and cancer [7][8][9][10][11] . Rab5 is indispensable at early endosomes 12 , where it has a role in the activation of VPS34 13 .…”

mentioning

confidence: 99%

Structural basis for VPS34 kinase activation by Rab1 and Rab5 on membranes

et al. 2021

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The lipid phosphatidylinositol-3-phosphate (PI3P) is a regulator of two fundamental but distinct cellular processes, endocytosis and autophagy, so its generation needs to be under precise temporal and spatial control. PI3P is generated by two complexes that both contain the lipid kinase VPS34: complex II on endosomes (VPS34/VPS15/Beclin 1/UVRAG), and complex I on autophagosomes (VPS34/VPS15/Beclin 1/ATG14L). The endosomal GTPase Rab5 binds complex II, but the mechanism of VPS34 activation by Rab5 has remained elusive, and no GTPase is known to bind complex I. Here we show that Rab5a–GTP recruits endocytic complex II to membranes and activates it by binding between the VPS34 C2 and VPS15 WD40 domains. Electron cryotomography of complex II on Rab5a-decorated vesicles shows that the VPS34 kinase domain is released from inhibition by VPS15 and hovers over the lipid bilayer, poised for catalysis. We also show that the GTPase Rab1a, which is known to be involved in autophagy, recruits and activates the autophagy-specific complex I, but not complex II. Both Rabs bind to the same VPS34 interface but in a manner unique for each. These findings reveal how VPS34 complexes are activated on membranes by specific Rab GTPases and how they are recruited to unique cellular locations.

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Host Cell Rab GTPases in Hepatitis B Virus Infection

Cited by 20 publications

References 79 publications

Efficient long-term amplification of hepatitis B virus isolates after infection of slow proliferating HepG2-NTCP cells

Efficient long-term amplification of hepatitis B virus isolates after infection of slow proliferating HepG2-NTCP cells

Efficient and reproducible depletion of hepatitis B virus from plasma derived extracellular vesicles

Structural basis for VPS34 kinase activation by Rab1 and Rab5 on membranes

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